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重组于脂质体中的人类有机阳离子转运体1(SLC22A4)催化乙酰胆碱转运,而与克罗恩病相关的突变体L503F存在该转运缺陷。

The human OCTN1 (SLC22A4) reconstituted in liposomes catalyzes acetylcholine transport which is defective in the mutant L503F associated to the Crohn's disease.

作者信息

Pochini Lorena, Scalise Mariafrancesca, Galluccio Michele, Pani Giovambattista, Siminovitch Katherine A, Indiveri Cesare

机构信息

Department of Cell Biology, University of Calabria, Arcavacata di Rende, Italy.

出版信息

Biochim Biophys Acta. 2012 Mar;1818(3):559-65. doi: 10.1016/j.bbamem.2011.12.014. Epub 2011 Dec 21.

Abstract

The organic cation transporter (OCTN1) plays key roles in transport of selected organic cations, but understanding of its biological functions remains limited by restricted knowledge of its substrate targets. Here we show capacity of human OCTN1-reconstituted proteoliposomes to mediate uptake and efflux of [(3)H]acetylcholine, the Km of transport being 1.0mM with V(max) of 160nmol⋅mg(-1)protein⋅min(-1). OCTN1-mediated transport of this neurotransmitter was time-dependent and was stimulated by intraliposomal ATP. The transporter operates as uniporter but translocates acetylcholine in both directions. [(3)H]acetylcholine uptake was competitively inhibited by tetraethylammonium, γ-butyrobetaine and acetylcarnitine, and was also inhibited by various polyamines. Decreasing intraliposomal ATP concentrations increased OCTN Km for acetylcholine, but V(max) was unaffected. Evaluation of the acetylcholine transporter properties of a variant form of OCTN1, the Crohn's disease-associated 503F variant, revealed time course, Km and V(max) for acetylcholine uptake to be comparable to that of wild-type OCTN1. Km for acetylcholine efflux was also comparable for both OCTN1 species, but V(max) of OCTN1 503F-mediated acetylcholine efflux (1.9nmol⋅mg(-1)protein⋅min(-1)) was significantly lower than that of wild-type OCTN1 (14nmol⋅mg(-1)protein⋅min(-1)). These data identify a new transport role for OCTN1 and raise the possibility that its involvement in the non-neuronal acetylcholine system may be relevant to the pathogenesis of Crohn's disease.

摘要

有机阳离子转运体(OCTN1)在特定有机阳离子的转运中起关键作用,但由于对其底物靶点的了解有限,对其生物学功能的认识仍然不足。在此,我们展示了重组人OCTN1的蛋白脂质体介导[³H]乙酰胆碱摄取和外排的能力,转运的Km为1.0 mM,V(max)为160 nmol·mg⁻¹蛋白质·min⁻¹。OCTN1介导的这种神经递质转运具有时间依赖性,并受到脂质体内ATP的刺激。该转运体作为单向转运体起作用,但能使乙酰胆碱双向转运。[³H]乙酰胆碱的摄取受到四乙铵、γ-丁酸甜菜碱和乙酰肉碱的竞争性抑制,也受到各种多胺的抑制。降低脂质体内ATP浓度会增加OCTN对乙酰胆碱的Km,但V(max)不受影响。对OCTN1的一种变体形式(与克罗恩病相关的503F变体)的乙酰胆碱转运特性进行评估,发现其摄取乙酰胆碱的时间进程、Km和V(max)与野生型OCTN1相当。两种OCTN1变体的乙酰胆碱外排Km也相当,但OCTN1 503F介导的乙酰胆碱外排的V(max)(1.9 nmol·mg⁻¹蛋白质·min⁻¹)显著低于野生型OCTN1(14 nmol·mg⁻¹蛋白质·min⁻¹)。这些数据确定了OCTN1的一种新的转运作用,并提出其参与非神经元乙酰胆碱系统可能与克罗恩病的发病机制有关的可能性。

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